2010
DOI: 10.1371/journal.pone.0013637
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MicroRNAs Are Mediators of Androgen Action in Prostate and Muscle

Abstract: Androgen receptor (AR) function is critical for the development of male reproductive organs, muscle, bone and other tissues. Functionally impaired AR results in androgen insensitivity syndrome (AIS). The interaction between AR and microRNA (miR) signaling pathways was examined to understand the role of miRs in AR function. Reduction of androgen levels in Sprague-Dawley rats by castration inhibited the expression of a large set of miRs in prostate and muscle, which was reversed by treatment of castrated rats wi… Show more

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Cited by 52 publications
(55 citation statements)
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“…It was also hypothesised that reduced AR function upon loss of androgen-stimulated miR synthesis may be a result of androgen-regulated miR targeting of AR corepressors. Consistent with this, 75% of predicted NCoR or SMRTtargeting miRs were upregulated in the prostate by DHT, and Dicer siRNA treatment increased transcription of both NCoR and SMRT (Narayanan et al 2010). Taken together, these innovative data identify androgen-responsive tissuespecific miR profiles, and confirm androgen-upregulated miRs as vital mediators and enhancers of AR signalling through corepressor targeting (discussed also below).…”
Section: Androgen Regulation Of Mir Biogenesissupporting
confidence: 64%
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“…It was also hypothesised that reduced AR function upon loss of androgen-stimulated miR synthesis may be a result of androgen-regulated miR targeting of AR corepressors. Consistent with this, 75% of predicted NCoR or SMRTtargeting miRs were upregulated in the prostate by DHT, and Dicer siRNA treatment increased transcription of both NCoR and SMRT (Narayanan et al 2010). Taken together, these innovative data identify androgen-responsive tissuespecific miR profiles, and confirm androgen-upregulated miRs as vital mediators and enhancers of AR signalling through corepressor targeting (discussed also below).…”
Section: Androgen Regulation Of Mir Biogenesissupporting
confidence: 64%
“…The miR profile was not altered in the liver upon androgen treatment, but the levator ani muscle (which has an anabolic response to androgens) demonstrated an upregulated miR profile that differed significantly from that of the prostate, preferentially targeting components of the Raf/MEK/ERK signalling pathway (Narayanan et al 2010). Interestingly, Dicer siRNA completely inhibited dihydrotestosterone (DHT) induction of the wellcharacterised androgen-responsive gene PSA in LNCaP cells, and Dicer K/K mice developed androgen-insensitivity syndrome, indicating that androgen-regulated miRs are vital mediators of AR action in vivo (Narayanan et al 2010). It was also hypothesised that reduced AR function upon loss of androgen-stimulated miR synthesis may be a result of androgen-regulated miR targeting of AR corepressors.…”
Section: Androgen Regulation Of Mir Biogenesismentioning
confidence: 94%
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“…Given that the miRNA transcriptome is profoundly affected by androgen signaling in PCa (for review, see Coppola et al (2009)), it is not surprising that androgenic regulation of many of the circulating miRNAs described earlier has been documented (e.g. miR-141 and other miR-200 family members (Szczyrba et al 2010, Waltering et al 2010, miR-375 (Szczyrba et al 2010, Waltering et al 2010, miR-21 (Shi et al 2007, Ribas et al 2009, Narayanan et al 2010, and miR-221 (Sun et al 2009)). These observations provide important mechanistic information regarding the origins of these potential biomarkers, which may be critical for their effective clinical implementation.…”
Section: Association Between Androgen Signaling and Circulating Mirnamentioning
confidence: 99%
“…Воздействие андрогенов на биогенез и функции микроРНК в рамках проблемы рака предстательной железы В норме андрогены регулируют экспрессию ми-кроРНК в ткани предстательной железы, благодаря чему контролируются многие структурные и функци-ональные особенности клеток простаты [25]. За послед-ние годы проведен ряд исследований изменения про-филя экспрессии микроРНК в клетках РПЖ [26][27][28], что позволило продемонстрировать роль микроРНК в опосредовании проканцерогенных эффектов андро-генов [29].…”
Section: том 2 обзорные статьиunclassified